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Descripción: Green tea has shown the role of chemoprevention for cancer. Recently, several studies suggested that green tea intake may have effect on esophageal cancer risk, whereas the results were inconsistent.

1471-230X Research article 23 February 2012 29 October 2012 21 November 2012 http://www.biomedcentral.com/1471-230X/12/165

Like all articles in BMC journals, this peer-reviewed article can be downloaded, printed and distributed freely for any purposes (see copyright notice below). Articles in BMC journals are listed in PubMed and archived at PubMed Central. For information about publishing your research in BMC journals or any BioMed Central journal, go to http://www.biomedcentral.com/info/authors/

Abstract
Background
Green tea has shown the role of chemoprevention for cancer. Recently, several studies suggested that green tea intake may have effect on esophageal cancer risk, whereas the results were inconsistent.

Methods
We performed a meta-analysis of all English and Chinese language studies of green tea consumption and esophageal cancer risk indexed in Medline, Embase, the Science Citation Index, the Chinese Biomedical Database and Wanfang Data from 1980 to June 2012. After reviewing each study, extracting data, and evaluating heterogeneity (Chi-square-based Q test and Ι2) and publication bias (Begg and Egger test), a meta-analysis was performed to evaluate the association between high/medium/low green tea consumption and non-drinking esophageal cancer risk. Pooled relative risk (RR) or odds ratio (OR) with 95% confidence intervals (CIs) were calculated using the fixed- or random-effect models.

Results
Ten eligible epidemiologic studies including 33731 participants and 3557 cases for esophageal cancer were included. Eight of which were case–control studies, and two were cohort studies. Overall, there were no association between high/medium/low green tea

Conclusions
We did not found significant association between green tea consumption and non-drinking esophageal cancer risk, but an evidence of protective effect was observed among female.

Background
Esophageal cancer is a major concern in the world, ranking the sixth most common cause of cancer mortality [1]. Lifestyles such as cigarettes smoking, alcohol drinking and dietary habits have been suggested to be associated with the carcinogenesis of esophageal cancer [2,3]. Tea is one of the most widely consumed beverages in the world [4]. Tea is divided into three major types: green tea (non-fermented), oolong tea (half-fermented) and black tea (fermented) according to on the manufacturing process. Green tea and its constituents such as epigallocatechin-3 gallate (EGCG), epigallocatechin (EGC) and epicatechin-3 gallate (ECG) have been shown to inhibit tumorigenesis in many animal models [5,6]. There have been a number of epidemiologic studies evaluated the relation between green tea intake and esophageal cancer risk in human, but with different results. Two large case–control studies [7,8] showed the protective effect of green tea intake on esophageal cancer incidence. However, another case–control study including 883 cases showed that people who have more consumption of green tea more susceptible to esophageal cancer [9]. No quantitative attempt has been to summarize the results of studies exploring a possible association between green tea and esophageal cancer. Therefore, we conducted this meta-analysis to examine the association in epidemiologic studies.

Methods
Search strategy
The electronic databases, Medline (1966 to June 2012), Embase (1980 to June 2012), the Science Citation Index (1945 to June 2012), the Chinese Biomedical Database (1981 to June 2012) and Wanfang Data (1980 to June 2012) were searched for epidemiologic studies published in English or Chinese of green tea intake in relation to esophageal cancer risk. We used the search terms “tea”, “food”, “diet”, “beverage”, “drinking” or “tea polyphenol” combined with “esophageal”, “oesophageal”, or “esophagus”. Firstly, the title and abstract of identified relevant studies were used to exclude any obviously irrelevant studies. The fulltexts and tables of the remaining articles were retrieved and perused to determine the relevancy of the study design and data, according to the inclusion criteria detailed below. Additional studies were identified by screening the reference lists of each relevant study. Furthermore, reviews concerning the relevant topic were retrieved from the above-mentioned

databases in order to potentially broaden the search by identifying additional relevant publications from the studies cited in the reviews.

Inclusion criteria
The following inclusion criteria were used to select relevant studies for the meta-analysis: (a) human studies, not laboratory or animal studies were included; (b) the daily consumption of the natural green tea product, not of green tea extracts or supplements were recorded; (c) the outcome of interest had to be an incidence of esophageal cancer; (d) relative risk (RR) or odds ratio (OR) estimates with corresponding 95% CIs (or sufficient information to calculate them) were reported. If two or more studies used the same population resource or had overlapping subjects, only the study reporting the largest population was selected for inclusion in the meta-analysis.

Data extraction
Two reviewers (Ping Zheng and Haiming Zheng) independently performed the data extraction. Disagreements were resolved by reviewers (Deng and Zhang), and a consensus was reached for all data prior to meta-analysis. The following information was collected: the first author’s name, publication year, the country of origin, follow-up duration, gender, the number of participants (cases and cohort size), measurements of green tea consumption, relative risk (RR, which is a ratio of the exposed group and non-exposed group incidence rate and suitable for cohort/prospective study), or odds ratio estimates (OR, which is suitable for case–control studies), and their corresponding 95% confidence intervals (95% CIs). We treated them as two different studies when a study provided separate RR/OR estimates for men and women. If a study provided several RR/ORs, we extracted the RR/ORs reflecting the greatest degree of control for potential interaction factors. When a study provided RR/OR for both esophageal cancer and invasive esophageal cancer, we used the former due to getting more cases.

Statistical analysis
To evaluate the association between green tea consumption and risk of esophageal cancer, the RR/OR with 95% CIs were calculated using pooled data from the studies. Data pooling was carried out by using the fixed effects model (based on the Mantel-Haenszel method) or the random effects model (based on the Dersimonian and Laird method) [10,11] The random effects model was used if heterogeneity existed between the studies from which the data was extracted; otherwise, the fixed effects model was used. Statistical heterogeneity between studies was assessed with the Chi-square-based Q test and Ι2, and heterogeneity was considered significant when the two-tailed P value was less than 0.10 [12]. Ι2 was used to qualify variation in RR/OR that was attributable to heterogeneity [13]. Publication bias was estimated by using the Begg and Mazumdar adjusted rank correlation test and the Egger regression asymmetry test [14,15]. Finally, the statistical significance of the RR/OR was determined by using the Z test. Since the original data of tea consumption dose is nonlinear, we divided the level of consumption into high, medium and low groups. We calculated the highest/lowest level of tea consumption as high/low group to compare with the non-drinking when the original literature provided the group of tea-drinking dose. When there is no dose group, we use the drink group as highest/lowest level of tea consumption respectively. We calculated the drinking of tea

consumption as medium group to compare with the non-drinking when the original literature provided the group of tea-drinking. And when there is several dose groups, we use the combination as drink group. So we generated three group of tea intake: highest vs nondrinker, drinker vs non-drinker, lowest vs non-drinker. We performed meta-analysis for all the included studies, and then made subgroup analysis according to study design, country, participates source and gender. This work was conducted on the basis of MOOSE guidelines proposed by the Meta-Analysis of Observational Studies in Epidemiology group [16]. All P values are two-tailed. For all tests, P values < 0.10 are considered statistically significant, except for heterogeneity. All analysis was performed by the Stata version 11.0 software (Stata Corporation, College Station, Texas).

Meta-Analysis of Case–control studies
Eight case–control studies were included. Of which, two studies [7,18] presented the OR and CIs for female and male respectively, and one study for participates from two different areas. All of them were treated as two studies when analysed. In the meta-analysis, green tea consumption was found to be associated with a significantly lower risk of esophageal cancer in high group (RR/OR = 0.72, 95% CI: 0.45 to 0.98, Table

2). The P value of heterogeneity chi-squared test was < 0.01, and the corresponding I2 statistic was 76%, suggesting variability between studies. The P values for the Begg’s and the Egger’s tests were P = 0.07 and P = 0.02, respectively, suggesting the probability of publication bias. The results in Medium and low group were not statistically significant (respectively: RR/OR = 0.85, 95% CI: 0.67 to 1.02, Table 3. RR/OR = 0.82, 95% CI: 0.56 to 1.09, Table 4). The P value of heterogeneity chi-squared test were all < 0.01. The corresponding I2 statistic were 65%, 72%. The P value for the Begg’s test and Egger’s test were 0.03 and 0.02, 0.07 and 0.01, respectively.

Meta-Analysis of Cohort studies
Two cohort studies were included [17]. The association between green tea consumption and the risk of esophageal cancer were all not statistically significant (high/medium/low respectively: RR/OR = 1.67, 95% CI: 0.46 to 2.87, Table 2. RR/OR = 1.14, 95% CI: 0.46 to 2.87, Table 3. RR/OR = 0.96, 95% CI: 0.01 to 1.92, Table 4). The P value of heterogeneity chi-squared test were 0.90, 0.90 and 0.59, respectively. The corresponding I2 statistic were all 0.0%, indicating a low variability between studies. The P value for the Begg’s test and Egger’s test were 1.00 and not applicable, 0.26 and 0.17, 0.07 and 0.01, respectively.

Combined and Subgroup Analysis
Furthermore, we performed the combined analysis of case–control and cohort studies. The association between green tea consumption and non-drinking risk of esophageal cancer were not statistically significant in three group (High: RR/OR = 0.76, 95% CI: 0.49 to 1.02, Table 2. Medium: RR/OR = 0.86, 95% CI: 0.70 to 1.03, Table 3. Low: RR/OR = 0.83, 95% CI: 0.58 to 1.08, Table 4.). The P value of heterogeneity chi-squared test were all < 0.01. The corresponding I2 statistic were 73%, 56%, 66%, respectively. The P value for the Begg’s test and Egger’s test were 0.37 and 0.16, 0.24 and 0.22, 0.16 and 0.03, respectively. Overall, no association was found between green tea consumption and non-drinking risk of esophageal cancer. When stratified by country, we did not found association between green tea consumption and non-drinking risk of esophageal cancer in China, Japan and Northern Iran (Tables 2, 3, 4) When stratified by participates source, we found a significant association between high green tea consumption and non-drinking esophageal cancer risk among PCC (RR/OR = 0.71; 95% CI: 0.43-0.98, P < 0.01 for heterogeneity, I2 = 78%), but not the HCC (RR/OR = 0.92; 95% CI: 0.49-2.32, with only one study, Table 2). We did not found association between medium/low green tea consumption and non-drinking risk of esophageal cancer in PCC and HCC. There were two studies [7,18] provided gender-specific RR estimates and 95% CIs for the association between green tea consumption and esophageal cancer risk, therefore we also made stratified analysis by gender. The results of meta-analysis showed that there were significant association between high/medium/low green tea consumption and non-drinking risk of esophageal cancer among female (High: RR/OR = 0.32, 95% CI: 0.10 to 0.54, P =

Sensitivity analysis
Sensitivity analysis has been carried out by excluding one study from others step by step in each group. They did not alter the original results.

Discussion
Our meta-analysis of epidemiologic studies did not found significant association between high/medium/low green tea consumption and non-drinking esophageal cancer risk, while an evidence of protective effect was observed among female. However, there are only two cases of case–control in female studies which existed all in China, this result can lead to selection bias. In addition, the positive results are more easily published, making publication bias generated. All that makes worthy of further consideration about female results. If excluding these factors, some other reason should be considered of the impact among female. Sex hormone may be an explanation for why female experiencing significantly a lower risk of esophageal cancer when take high level green tea. A sex hormone-mediated pathway may be involved in esophageal carcinogenesis, which was supported by two experimental studies [22,23]. A suppressing effect of estrogen and a promoting effect of androgen were shown in the experimental induction of esophageal cancer by the administration of chemical carcinogen [22]. Meanwhile, the growth rate of metastatic squamous cell carcinoma of the esophagus was inhibited by estrogen and enhanced by testosterone, respectively [23]. Additional studies are warranted to explain and confirm this preliminary evidence. There have been a number of experimental and clinical studies suggesting drinking beverages at high temperatures to be a cause of esophageal cancer. The facts that more tumors were showed and larger size of esophagus papillomas were rapidly increased when the temperature at 70°C and above was reported by a previous experimental study [24]. In our meta-analysis, two included studies [9,19] both found that drinking tea at high temperature significantly increases risk of esophageal cancer incidence. However, the two studies had different definition for high or normal temperature of green tea drinking, which make it difficult to be stratified for further analysis. Three studies [9,17,19] included in the meta-analysis have investigated the effects of green tea drinking and dose response relationship. No dose–response relationship was observed among the two studies [17,19]. In the study conducted by Wu [9], higher monthly consumption of tea (P for trend = 0.07) and usually drinking tea in high concentration (P for trend = 0.01) showed a positive tendency with cancer risk for ever drinker after adjusting for tea temperature. We have analysised data by grouping high/medium/low intake. However, we have not found it is effective between green tea consumption and non-drinking in esophageal cancer risk.

The protective effect of high green tea consumption on esophageal cancer was observed among case–control studies and PCC, but both the heterogeneity and publication bias are significant. So the protective effect among case–control studies and PCC may be incredible. Furthermore we performed the combined analysis of case–control and cohort studies. The heterogeneity and publication bias are not significant in the overall study. So, there may be no significant association between high green tea consumption and non-drinking esophageal cancer risk in the meta-analysis. Focus on heterogeneity and publication bias of the analyses, we found all the estimates with several studies with a large sample size are very heterogeneous, while estimates with a couple of studies and small sample size have no heterogeneity. For example, both meta-analyses of all studies (ten studies) and case–control studies (eight studies), the P for heterogeneity were < 0.01, suggesting variability between studies. However, for meta-analyses among female (two studies) or male (two studies), the P for heterogeneity were both > 0.05, suggesting a low variability between studies. When heterogeneity existed we used the random effects model to adjusted. The publication bias among case–control and PCC studies are significant in high group. The cautions for above phenomenon may be as follows: (a) Most of case– control and population-based case–control studies were performed among China [7-9,18-21], and that may cause bias. (b) Retrospective bias. (c) Positive results may be publicated more easily. Furthermore, we performed subgroup analysis by sex, geographic region and type of epidemiologic studies. However, there are several disadvantages should be considered in our meta-analysis. First, publication bias in China studies or case control studies cannot be missed. The protective effect of green tea in female may be misled by a publication bias because of the female studies all from China studies or case control studies. Second, the epidemiologic studies were not much enough to be stratified for dose and temperature of green tea intake, which may mitigate the result. Third, the non-English and non-Chinese literature could not be reviewed because of the language barrier. Last, most of the studies included in the analysis had been conducted among Asian populations due to popularity of green tea in East Asia. Therefore, the results should be cautious extrapolated to other populations.

Conclusions
The results of our meta-analysis did not found significant association between green tea consumption and non-drinking esophageal cancer risk, but an evidence of protective effect was observed among female. Additional more studies (especial the cohort studies, and studies from more countries) with careful control of interaction factors including dose and temperature of green tea intake are needed to provide a more definitive conclusion focusing on whether the routine consumption of green tea can guard against esophageal cancer.

Competing interests
The authors declare that they have no competing interests.

Authors’ contributions
PZ and HMZ carried out the literature search, selection, validity, assessment, data abstraction and data analysis respectively. PZ and HMZ wrote the paper. XMD and YDZ had the original idea for the paper and revision of the article. All authors reviewed and approved the final draft of the paper.

Acknowledgements
Declaration of personal interests: we are indebted to the authors of the primary studies.